Comparative effects of cyclo‐oxygenase and nitric oxide synthase inhibition on the development and reversal of spinal opioid tolerance

Powell, Kelly J.; Hosokawa, Akiko; Bell, Andrew; Sutak, Maaja; Milne, Brian; Quirion, Rémi; Jhamandas, Khem

doi:10.1038/sj.bjp.0702587

Cited by 88 publications

(66 citation statements)

References 39 publications

(59 reference statements)

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“…The role of these mediators in the development of morphine tolerance and opioid withdrawal-induced hyperalgesia is well documented (Mao et al, 1995;Powell et al, 1999;Raghavendra et al, 2002). In the present study, we observed that the propentofylline attenuation of morphine tolerance and its withdrawal-induced hyperalgesia was also associated with decreased spinal proinflammatory immune responses.…”

Section: Mechanisms For Morphine-induced Glial Activationsupporting

confidence: 67%

Attenuation of Morphine Tolerance, Withdrawal-Induced Hyperalgesia, and Associated Spinal Inflammatory Immune Responses by Propentofylline in Rats

Raghavendra

Tanga

DeLeo

2003

Neuropsychopharmacol

225

175

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The activation of glial cells and enhanced proinflammatory cytokine expression at the spinal cord has been implicated in the development of morphine tolerance, and morphine withdrawal-induced hyperalgesia. The present study investigated the effect of propentofylline, a glial modulator, on the expression of analgesic tolerance and withdrawal-induced hyperalgesia in chronic morphine-treated rats. Chronic morphine administration through repeated subcutaneous injection induced glial activation and enhanced proinflammatory cytokine levels at the lumbar spinal cord. Moreover, glial activation and enhanced proinflammatory cytokine levels exhibited a temporal correlation with the expression of morphine tolerance and hyperalgesia. Consistently, propentofylline attenuated the development of hyperalgesia and the expression of spinal analgesic tolerance to morphine. The administration of propentofylline during the induction of morphine tolerance also attenuated glial activation and proinflammatory cytokines at the L5 lumbar spinal cord. These results further support the hypothesis that spinal glia and proinflammatory cytokines contribute to the mechanisms of morphine tolerance and associated abnormal pain sensitivity.

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Section: Mechanisms For Morphine-induced Glial Activationsupporting

confidence: 67%

Attenuation of Morphine Tolerance, Withdrawal-Induced Hyperalgesia, and Associated Spinal Inflammatory Immune Responses by Propentofylline in Rats

Raghavendra

Tanga

DeLeo

2003

Neuropsychopharmacol

225

175

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“…As was observed in our previous studies (Mendard et al, 1996), CGRP 8-37 inhibited the development of morphine tolerance, and this eect was mimicked by BIBN4096BS. The action of CGRP receptor blockade on the development of tolerance to spinal morphine was not due to a potentiation of acute morphine action, or a sensitization to morphine as was previously observed with the NMDA receptor antagonist MK801 (Dunbar & Yaksh, 1996) or inhibitors of cyclooxygenase activity like ketorolac and ibuprofen (Powell et al, 1999). In fact, BIBN4096BS slightly inhibited the acute antinociceptive action of morphine in the tail-¯ick test but still attenuated the loss of morphine potency associated with chronic treatment.…”

Section: Discussionmentioning

confidence: 60%

“…Thus, an increase in substance P activity could reduce the ability of opioids to inhibit transmitter release and produce antinociception. We have recently shown that intrathecal application of prostanoid synthesis inhibitors eectively blocks and reverses the development of opioid tolerance (Powell et al, 1999). Our preliminary ®ndings with a substance P receptor antagonist (SR140333) have also revealed its potential to inhibit spinal morphine tolerance (Powell et al, 1999, unpublished results).…”

Section: Discussionmentioning

confidence: 91%

“…Previous experiments have shown that established tolerance can be reversed by pharmacological manipulation of NMDA receptor activity with antagonists such as ketamine and LY274614 (Tiseo & Inturrisi, 1993;Elliott et al, 1994;Shimoyama et al, 1996). Additionally, the inhibition of the production of intermediaries of NMDA receptor activity (prostaglandins and nitric oxide) also reverses established tolerance (Kolesnikov et al, 1993;Powell et al, 1999). Since CGRP can release Lglutamate (Kangrga et al, 1990) and enhance NMDA receptor-mediated excitation (Murase et al, 1989), it is likely that CGRP also contributes to the maintenance of tolerance.…”

Section: Introductionmentioning

confidence: 99%

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Blockade and reversal of spinal morphine tolerance by peptide and non‐peptide calcitonin gene‐related peptide receptor antagonists

Powell

Sutak

et al. 2000

British J Pharmacology

Self Cite

108

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1 This study examined the eects of the peptide CGRP receptor antagonist CGRP and the newly-developed non-peptide CGRP receptor antagonist BIBN4096BS for their potential to both inhibit the development and reverse tolerance to the antinociceptive action of morphine. 2 Repeated administration of intrathecal morphine (15 mg), once daily, produced a progressive decline of antinociceptive eect and an increase in the ED 50 value in the tail¯ick and paw pressure tests. Co-administration of CGRP 8-37 (4 mg) or BIBN4096BS (0.05, 0.1 mg) with morphine (15 mg) prevented the decline of antinociceptive eect and increase in ED 50 value in the tail¯ick test. Intrathecal administration of the CGRP receptor antagonists did not alter the baseline responses in either tests. Acute CGRP 8-37 also did not potentiate the acute actions of spinal morphine. 3 In animals rendered tolerant to intrathecal morphine, subsequent administration of CGRP (4 mg) with morphine (15 mg) partially restored the antinociceptive eect and ED 50 value of acute morphine, re¯ecting the reversal of tolerance. 4 Animals tolerant to intrathecal morphine expressed increased CGRP and substance P-like immunostaining in the dorsal horn of the spinal cord. The increase in CGRP, but not substance Plike immunostaining, was blocked by a co-treatment with CGRP 8-37 (4 mg). In animals already tolerant to morphine, the increase in CGRP but not substance P-like immunostaining was partially reversed by CGRP 8-37 (4 mg). 5 These data suggest that activation of spinal CGRP receptors contributes to both the development and expression of spinal opioid tolerance. CGRP receptor antagonists may represent a useful therapeutic approach for preventing as well as reversing opioid tolerance.

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“…Tolerance to the analgesic effect of opioids is believed to be mediated at least partly by prostaglandin-mediated mechanisms (Powell et al, 1999). Intrathecal administration of COX-2 inhibitors attenuates the development of tolerance to morphine (Wong et al, 2000).…”

Section: Discussionmentioning

confidence: 99%

COX-2 inhibitor celecoxib prevents chronic morphine-induced promotion of angiogenesis, tumour growth, metastasis and mortality, without compromising analgesia

et al. 2007

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Morphine and its congener opioids are the main therapy for severe pain in cancer. However, chronic morphine treatment stimulates angiogenesis and tumour growth in mice. We examined if celecoxib (a cyclooxygenase-2 (COX-2) inhibitor) prevents morphineinduced tumour growth without compromising analgesia. The effect of chronic treatment with celecoxib (by gavage) and/or morphine (subcutaneously), or PBS on tumour prostaglandin E 2 (PGE 2 ), COX-2, angiogenesis, tumour growth, metastasis, pain behaviour and survival was determined in a highly invasive SCK breast cancer model in A/J mice. Two weeks of chronic morphine treatment at clinically relevant doses stimulates COX-2 and PGE 2 (4.5-fold compared to vehicle alone) and angiogenesis in breast tumours in mice. This is accompanied by increased tumour weight (B35%) and increased metastasis and reduced survival. Coadministration of celecoxib prevents these morphine-induced effects. In addition, morphine and celecoxib together provided better analgesia than either agent alone. Celecoxib prevents morphine-induced stimulation of COX-2, PGE 2 , angiogenesis, tumour growth, metastasis and mortality without compromising analgesia in a murine breast cancer model. In fact, the combination provided significantly better analgesia than with morphine or celecoxib alone. Clinical trials of this combination for analgesia in chronic and severe pain in cancer are warranted.

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Comparative effects of cyclo‐oxygenase and nitric oxide synthase inhibition on the development and reversal of spinal opioid tolerance

Cited by 88 publications

References 39 publications

Attenuation of Morphine Tolerance, Withdrawal-Induced Hyperalgesia, and Associated Spinal Inflammatory Immune Responses by Propentofylline in Rats

Attenuation of Morphine Tolerance, Withdrawal-Induced Hyperalgesia, and Associated Spinal Inflammatory Immune Responses by Propentofylline in Rats

Blockade and reversal of spinal morphine tolerance by peptide and non‐peptide calcitonin gene‐related peptide receptor antagonists

COX-2 inhibitor celecoxib prevents chronic morphine-induced promotion of angiogenesis, tumour growth, metastasis and mortality, without compromising analgesia

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